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HIV-1感染后针对gp41、p24和p17的IgG抗体亲和力的差异成熟

Differential maturation of avidity of IgG antibodies to gp41, p24 and p17 following infection with HIV-1.

作者信息

Thomas H I, Wilson S, O'Toole C M, Lister C M, Saeed A M, Watkins R P, Morgan-Capner P

机构信息

Department of Virology, Royal Preston Hospital, UK.

出版信息

Clin Exp Immunol. 1996 Feb;103(2):185-91. doi: 10.1046/j.1365-2249.1996.951642.x.

Abstract

We have evaluated solid-phase ELISA IgG antibody avidity studies as a means of identifying cases of recent HIV-1 infection. Although separate studies on the avidity of anti-gp41 and anti-p24 antibodies in seroconvertors have been reported, a comparison of the ability of patients to simultaneously mature their immune response to more than one HIV antigen immediately following seroconversion appears to be lacking. We have demonstrated a maturation in anti-gp41 avidity which reflects the time since seroconversion in all cases. In contrast, however, only some patients produced high-avidity anti-p24 or anti-p17 antibodies during the same time span. While the avidity of anti-gp41 antibodies remained high in cases of non-recent HIV infection, even in the face of advanced disease, we have confirmed the findings of others that the avidity of anti-p24 falls before the onset of ARC or AIDS. Therefore, whilst the avidity of anti-gp41 antibodies could reliably be of value in identifying cases of recent HIV infection, the avidity of anti-p24 or anti-p17 antibodies could not, but may be of prognostic value, even at an early stage. The time taken to reach maximum anti-p17, anti-p24 and anti-gp41 titres was variable, but anti-gp41 titres, like anti-gp41 avidity, remained high. In contrast, anti-p24 titres fell, even during the early followup period in some seroconvertors. Anti-p24 antibody avidity, however, appeared to be a better predictor of disease progression in 'remote' cases than anti-p24 titre. The avidity and titres of these antibodies are presented in relation to the clinical details, p24 antigen status, CD4 and CD8 counts where these are known.

摘要

我们评估了固相ELISA IgG抗体亲和力研究,以此作为识别近期HIV-1感染病例的一种方法。尽管已有关于血清转化者中抗gp41和抗p24抗体亲和力的单独研究报道,但似乎缺乏对患者在血清转化后立即同时成熟其针对多种HIV抗原的免疫反应能力的比较。我们已经证明,抗gp41亲和力的成熟反映了所有病例中血清转化后的时间。然而,相比之下,只有一些患者在同一时间段内产生了高亲和力的抗p24或抗p17抗体。在非近期HIV感染的病例中,即使面对晚期疾病,抗gp41抗体的亲和力仍然很高,我们已经证实了其他人的发现,即抗p24的亲和力在ARC或AIDS发作前下降。因此,虽然抗gp41抗体的亲和力在识别近期HIV感染病例中可能具有可靠价值,但抗p24或抗p17抗体的亲和力则不然,但即使在早期阶段,可能具有预后价值。达到抗p17、抗p24和抗gp41最高滴度所需的时间各不相同,但抗gp41滴度,就像抗gp41亲和力一样,仍然很高。相比之下,抗p24滴度下降,甚至在一些血清转化者的早期随访期间也是如此。然而,在“远期”病例中,抗p24抗体亲和力似乎比抗p24滴度更能预测疾病进展。这些抗体的亲和力和滴度与已知的临床细节、p24抗原状态、CD4和CD8计数相关呈现。

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